Development of a primary tamarin hepatocyte culture system for GB virus-B: a surrogate model for hepatitis C virus

被引:56
|
作者
Beames, B
Chavez, D
Guerra, B
Notvall, L
Brasky, KM
Lanford, RE
机构
[1] SW Fdn Biomed Res, Dept Virol & Immunol, SW Reg Primate Res Ctr, San Antonio, TX 78227 USA
[2] SW Fdn Biomed Res, Dept Lab Anim Med, SW Reg Primate Res Ctr, San Antonio, TX 78227 USA
关键词
D O I
10.1128/JVI.74.24.11764-11772.2000
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
GB virus-B (GBV-B) causes an acute hepatitis in tamarins characterized by increased alanine transaminase levels that quickly return to normal as the virus is cleared. Phylogenetically, GBV-B is the closest relative to hepatitis C virus (HCV), and thus GBV-B infection of tamarins represents a powerful surrogate model system for the study of HCV. In this study, the course of infection of GBV-B in tamarins was followed using a real-time 5 ' exonuclease (TaqMan) reverse transcription-PCR assay to determine the level of GBV-B in the serum. Peak viremia levels exceeded 10(9) genome equivalents/ml, followed by viral clearance within 14 to 16 weeks. Rechallenge of animals that had cleared infection resulted in viremia that was limited to 1 week, suggestive of a strong protective immune response. A robust tissue culture system for GBV-B was developed using primary cultures of tamarin hepatocytes. Hepatocytes obtained from a GBV-B-infected animal maintained high levels of cell-associated viral RNA and virion secretion for 42 days of culture. In vitro infection of normal hepatocytes resulted in rapid amplification of cell-associated viral RNA and secretion of up to 10(7) genome equivalents/ml of culture supernatant. In addition, infection could be monitored by immunofluorescence staining for GBV-B nonstructural NS3 protein. This model system overcomes many of the current obstacles to HCV research, including low levels of viral replication, lack of a small primate animal model, and lack of a reproducible tissue culture system.
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页码:11764 / 11772
页数:9
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